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脾切除术对经抗淋巴细胞血清处理并注射骨髓的小鼠诱导产生的对皮肤同种异体移植的特异性无反应性的影响。

Effect of splenectomy on specific unresponsiveness to skin allografts induced in ALS-treated, marrow-injected mice.

作者信息

Wood M L, Gottschalk R, Monaco A P

出版信息

Transplantation. 1980 Apr;29(4):320-3. doi: 10.1097/00007890-198004000-00012.

Abstract

The role of the spleen in the induction and maintenance of unresponsiveness to skin allografts and in the generation of suppressor cells has been studied in ALS-treated B6AF1 mice grafted with C3H/He skin and injected with C3H/He marrow. B6AF1 mice were splenectomized either before the induction of unresponsiveness or on day +13, +28, or +42 after unresponsiveness was induced. Graft survival in the splenectomized mice was compared to that observed in nonsplenectomized ALS-treated, marrow-injected controls. Graft survival was prolonged equally in all splenectomized groups and the nonsplenectomized controls. To study the effect of the spleen on the generation of suppressor cells, lymph node cells were removed at day +42 from splenectomized ALS-treated, marrow-injected B6AF1 mice bearing C3H/He skin grafts and transferred to ALS-treated B6AF1 recipientso ALS-treated BTAF1 recipients grafted with C3H/He skin. Graft survival in the secondary recipients receiving lymph node cells from splenectomized donors was compared to that observed in ALS-treated B6AF1 mice that received lymph node cells transferred from nonsplenectomized enhanced donors. Suppressor cell activity could be detected in the nodes of splenectomized mice, but a higher dose of lymph node cells was required to transfer unresponsiveness from splenectomized donors compared to nonsplenectomized donors. These results indicate that the spleen is not necessary for the induction or maintenance of unresponsiveness to skin allografts in ALS-treated, marrow-injected mice. In addition, suppressor cells can be generated in the lymph nodes of unresponsive mice in the absence of the spleen, although the production of suppressor cells appears to be less effective in splenectomized mice than in mice with intact spleens.

摘要

在经抗淋巴细胞血清(ALS)处理并移植C3H/He皮肤且注射C3H/He骨髓的B6AF1小鼠中,研究了脾脏在诱导和维持对皮肤同种异体移植物无反应性以及在产生抑制细胞方面的作用。B6AF1小鼠在诱导无反应性之前或在诱导无反应性后的第13、28或42天进行脾切除。将脾切除小鼠的移植物存活情况与未进行脾切除、经ALS处理且注射骨髓的对照小鼠的情况进行比较。所有脾切除组和未进行脾切除的对照组的移植物存活时间均同等延长。为了研究脾脏对抑制细胞产生的影响,在第42天从经脾切除、经ALS处理、注射骨髓且带有C3H/He皮肤移植物的B6AF1小鼠中取出淋巴结细胞,并将其转移至经ALS处理的B6AF1受体小鼠或移植有C3H/He皮肤的经ALS处理的BTAF1受体小鼠。将接受来自脾切除供体的淋巴结细胞的二次受体中的移植物存活情况与接受来自未进行脾切除的增强供体转移的淋巴结细胞的经ALS处理的B6AF1小鼠中的情况进行比较。在脾切除小鼠的淋巴结中可检测到抑制细胞活性,但与未进行脾切除的供体相比,需要更高剂量的淋巴结细胞才能从脾切除供体转移无反应性。这些结果表明,在经ALS处理、注射骨髓的小鼠中,脾脏对于诱导或维持对皮肤同种异体移植物的无反应性并非必需。此外,在无脾脏的情况下,无反应小鼠的淋巴结中可产生抑制细胞,尽管脾切除小鼠中抑制细胞的产生似乎比脾脏完整的小鼠效果要差。

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